Jan C Kamp, Omid Madadi-Sanjani, Marie Uecker, Christopher Werlein, Lavinia Neubert, Joachim F Kübler, Mikal Obed, Norman Junge, Tobias Welte, Jannik Ruwisch, Danny D Jonigk, Jan Stolk, Gertrud Vieten, Sabina Janciauskiene
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Transcriptome profiles were assessed using a panel of 768 fibrosis-specific genes, reanalyzed via qRT-PCR, and confirmed via immunostaining. Plasma from an additional 30 BA infants and 10 age-matched controls were used for amyloid precursor protein (APP) quantification by ELISA.</p><p><strong>Results: </strong>Different clinical outcome groups showed a homogeneous mRNA expression. Altered amyloid-metabolism-related gene expression was found between cases with Ishak fibrosis score greater than 4. Immunostaining confirmed a distinct presence of APP in the livers of all BA subjects. APP plasma levels were higher in BA than in age-matched controls and correlated with the histological fibrosis grade.</p><p><strong>Conclusions: </strong>These results suggest that amyloidosis may contribute to BA and liver fibrosis, indicating that APP could serve as a potential liquid biomarker for these conditions.</p><p><strong>Impact: </strong>Biliary atresia patients with higher fibrosis scores according to Ishak have higher hepatic expression of amyloid-related genes while amyloid precursor protein accumulates in the liver and increases in the circulation. After a recent study revealed beta-amyloid deposition as a mechanism potentially involved in biliary atresia, we were able to correlate amyloid-metabolism-related transcript levels as well as amyloid precursor protein tissue and plasma levels with the degree of hepatic fibrosis. These findings suggest that amyloid precursor protein is a fibrosis marker in infants with biliary atresia, reinforcing the role of amyloid metabolism in the pathogenesis of this serious disease.</p>","PeriodicalId":19829,"journal":{"name":"Pediatric Research","volume":null,"pages":null},"PeriodicalIF":3.1000,"publicationDate":"2024-09-28","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Amyloid precursor protein as a fibrosis marker in infants with biliary atresia.\",\"authors\":\"Jan C Kamp, Omid Madadi-Sanjani, Marie Uecker, Christopher Werlein, Lavinia Neubert, Joachim F Kübler, Mikal Obed, Norman Junge, Tobias Welte, Jannik Ruwisch, Danny D Jonigk, Jan Stolk, Gertrud Vieten, Sabina Janciauskiene\",\"doi\":\"10.1038/s41390-024-03582-w\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background: </strong>Biliary atresia (BA) is a rare condition of unknown origin in newborns with jaundice. 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引用次数: 0
摘要
背景:胆道闭锁(BA)是新生儿黄疸中一种原因不明的罕见疾病。胆道闭锁导致新生儿胆汁淤积,继而引起肝纤维化和肝功能衰竭:这项回顾性研究包括 14 名 BA 婴儿的肝脏活组织切片,他们的年龄为 [平均值 ± SD] 63 ± 23 天。根据临床过程(无黄疸 vs 复发性黄疸 vs 需要肝移植或肝纤维化(Ishak 纤维化评分))对患者进行分组,并随访 1.61-5.64 年(平均 4.03 年)。使用 768 个纤维化特异性基因组成的小组评估转录组概况,通过 qRT-PCR 进行再分析,并通过免疫染色法进行确认。另外 30 名 BA 婴儿和 10 名年龄匹配的对照组的血浆被用于通过 ELISA 对淀粉样前体蛋白(APP)进行定量:结果:不同的临床结果组显示出相同的 mRNA 表达。免疫染色证实所有 BA 受试者的肝脏中都明显存在 APP。BA患者的血浆中APP水平高于年龄匹配的对照组,并与组织学纤维化等级相关:这些结果表明,淀粉样变性可能是导致胆汁淤积症和肝纤维化的原因之一,表明APP可作为这些疾病的潜在液体生物标志物:影响:根据 Ishak 标准,纤维化评分较高的胆道闭锁患者肝脏中淀粉样蛋白相关基因的表达量较高,同时淀粉样蛋白前体在肝脏中积累,并在血液循环中增加。最近的一项研究表明,β-淀粉样蛋白沉积是胆道闭锁可能涉及的一种机制,此后,我们将淀粉样蛋白代谢相关转录物水平以及淀粉样前体蛋白组织和血浆水平与肝纤维化程度联系起来。这些发现表明,淀粉样前体蛋白是胆道闭锁婴儿肝纤维化的标志物,从而加强了淀粉样蛋白代谢在这种严重疾病发病机制中的作用。
Amyloid precursor protein as a fibrosis marker in infants with biliary atresia.
Background: Biliary atresia (BA) is a rare condition of unknown origin in newborns with jaundice. In BA bile ducts are non-functional, causing neonatal cholestasis and following liver fibrosis and failure.
Methods: This retrospective study included liver biopsies of 14 infants with BA aged [mean ± SD] 63 ± 23 days. Patients were grouped according to the clinical course (jaundice-free vs recurrent jaundice vs required liver transplantation or liver fibrosis (Ishak fibrosis score)) and followed for 1.61-5.64 years (mean 4.03). Transcriptome profiles were assessed using a panel of 768 fibrosis-specific genes, reanalyzed via qRT-PCR, and confirmed via immunostaining. Plasma from an additional 30 BA infants and 10 age-matched controls were used for amyloid precursor protein (APP) quantification by ELISA.
Results: Different clinical outcome groups showed a homogeneous mRNA expression. Altered amyloid-metabolism-related gene expression was found between cases with Ishak fibrosis score greater than 4. Immunostaining confirmed a distinct presence of APP in the livers of all BA subjects. APP plasma levels were higher in BA than in age-matched controls and correlated with the histological fibrosis grade.
Conclusions: These results suggest that amyloidosis may contribute to BA and liver fibrosis, indicating that APP could serve as a potential liquid biomarker for these conditions.
Impact: Biliary atresia patients with higher fibrosis scores according to Ishak have higher hepatic expression of amyloid-related genes while amyloid precursor protein accumulates in the liver and increases in the circulation. After a recent study revealed beta-amyloid deposition as a mechanism potentially involved in biliary atresia, we were able to correlate amyloid-metabolism-related transcript levels as well as amyloid precursor protein tissue and plasma levels with the degree of hepatic fibrosis. These findings suggest that amyloid precursor protein is a fibrosis marker in infants with biliary atresia, reinforcing the role of amyloid metabolism in the pathogenesis of this serious disease.
期刊介绍:
Pediatric Research publishes original papers, invited reviews, and commentaries on the etiologies of children''s diseases and
disorders of development, extending from molecular biology to epidemiology. Use of model organisms and in vitro techniques
relevant to developmental biology and medicine are acceptable, as are translational human studies
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